Fig. 2.

Aberrant T-cell profile is responsible for impaired GC selection in lupus mice. (A and B) Representative image (A) and cell counts (B) of spleens from Ship^fl/fl, Ship^ΔB, and Ship^ΔGCB mice. (C–E) Representative FACS profile (C) and bar graph (D and E) showing the percentage of CD44⁺CD62L⁻ effector/memory cells (T_EM) among CD4⁺ (D) and CD8⁺ (E) T cells in the spleen of Ship^fl/fl and Ship^ΔB mice. (F–H) Representative FACS profile (F) and bar graph (G and H) showing the percentage (F and G) and absolute number (H) of T_FH cells in the spleen of Ship^fl/fl and Ship^ΔB mice analyzed 2 wk after NP-CGG immunization. (I) Immunofluorescence image of frozen sections of spleens from Ship^fl/fl mice and Ship^ΔB mice analyzed 2 wk after NP-CGG immunization. (J) Percentage of GCB cells (PNA⁺CD95⁺) in total spleen B cells of Ship^fl/fl or Ship^ΔB mice. (K–M) Percentage of T_EM cells among CD4⁺ (K and L) or CD8⁺ (M) T cells in the spleen of TMPD-induced mice (K) and Bm12 cGVHD mice (L and M). (N and O) Representative FACS profile (N) and bar graph (O) showing the percentage of T_FH cells in the spleen of Bm12 cGVHD mice 2 wk after NP-CGG immunization. (P and Q) Representative FACS profile (P) and bar graph (Q) showing the percentage of B1-8^hi cells among non-GC or GC B cells in T cell-deficient mice (TCRβ^−/−TCRδ^−/−) transplanted with T cells isolated from Ship^fl/fl, Ship^ΔB, or Ship^ΔBMyd88^ΔB mice and then treated and analyzed as in Fig. 1A. Each symbol in the bar graphs represents an individual mouse. Bars represent means ± SD. ns, not significant; *P ≤ 0.05; **P ≤ 0.01; ***P ≤ 0.001; ****P ≤ 0.0001 (1-way ANOVA with Sidak’s multiple comparisons test [B]; unpaired 2-tailed t test [D, G, H, J–M, and O], 2-way ANOVA with Sidak’s multiple comparisons test [Q]). A representative of 2 (L–O) or 3 (A–K) independent experiments is shown. Q is summarized from 2 independent experiments with similar results.